MRI-Based Digital Models Forecast Patient-Specific Treatment Responses to Neoadjuvant Chemotherapy in Triple-Negative Breast Cancer

医学 乳腺癌 环磷酰胺 三阴性乳腺癌 新辅助治疗 化疗 病态的 一致性 肿瘤科 内科学 紫杉醇 接收机工作特性 癌症 阿霉素 核医学 放射科
作者
Chengyue Wu,Angela M. Jarrett,Zijian Zhou,Nabil Elshafeey,Beatriz E. Adrada,Rosalind P. Candelaria,Rania M. Mohamed,Medine Böge,Lei Huo,Jason B. White,Debu Tripathy,Vicente Valero,Jennifer K. Litton,Clinton Yam,Jong Bum Son,Jingfei Ma,Gaiane M. Rauch,Thomas E. Yankeelov
出处
期刊:Cancer Research [American Association for Cancer Research]
卷期号:82 (18): 3394-3404 被引量:33
标识
DOI:10.1158/0008-5472.can-22-1329
摘要

Triple-negative breast cancer (TNBC) is persistently refractory to therapy, and methods to improve targeting and evaluation of responses to therapy in this disease are needed. Here, we integrate quantitative MRI data with biologically based mathematical modeling to accurately predict the response of TNBC to neoadjuvant systemic therapy (NAST) on an individual basis. Specifically, 56 patients with TNBC enrolled in the ARTEMIS trial (NCT02276443) underwent standard-of-care doxorubicin/cyclophosphamide (A/C) and then paclitaxel for NAST, where dynamic contrast-enhanced MRI and diffusion-weighted MRI were acquired before treatment and after two and four cycles of A/C. A biologically based model was established to characterize tumor cell movement, proliferation, and treatment-induced cell death. Two evaluation frameworks were investigated using: (i) images acquired before and after two cycles of A/C for calibration and predicting tumor status after A/C, and (ii) images acquired before, after two cycles, and after four cycles of A/C for calibration and predicting response following NAST. For Framework 1, the concordance correlation coefficients between the predicted and measured patient-specific, post-A/C changes in tumor cellularity and volume were 0.95 and 0.94, respectively. For Framework 2, the biologically based model achieved an area under the receiver operator characteristic curve of 0.89 (sensitivity/specificity = 0.72/0.95) for differentiating pathological complete response (pCR) from non-pCR, which is statistically superior (P < 0.05) to the value of 0.78 (sensitivity/specificity = 0.72/0.79) achieved by tumor volume measured after four cycles of A/C. Overall, this model successfully captured patient-specific, spatiotemporal dynamics of TNBC response to NAST, providing highly accurate predictions of NAST response.
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